Ubiquitination-dependent mechanisms regulate synaptic growth and function

DiAntonio, Aaron; Haghighi, A. Pejmun; Portman, Scott L.; Lee, Jason D.; Amaranto, Andrew M.; Goodman, Corey S.

doi:10.1038/35086595

Cited by 366 publications

(322 citation statements)

References 23 publications

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“…Overexpression of faf in the developing Drosophila nervous system causes synaptic overgrowth and perturbs synaptic transmission. A similar phenotype is observed when a yeast DUB is expressed in the fruit fly CNS (DiAntonio et al 2001).…”

Section: Dubssupporting

confidence: 67%

The ubiquitin-proteasome pathway and synaptic plasticity

Hegde¹

2010

Learn. Mem.

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Proteolysis by the ubiquitin-proteasome pathway (UPP) has emerged as a new molecular mechanism that controls wideranging functions in the nervous system, including fine-tuning of synaptic connections during development and synaptic plasticity in the adult organism. In the UPP, attachment of a small protein, ubiquitin, tags the substrates for degradation by a multisubunit complex called the proteasome. Linkage of ubiquitin to protein substrates is highly specific and occurs through a series of well-orchestrated enzymatic steps. The UPP regulates neurotransmitter receptors, protein kinases, synaptic proteins, transcription factors, and other molecules critical for synaptic plasticity. Accumulating evidence indicates that the operation of the UPP in neurons is not homogeneous and is subject to tightly managed local regulation in different neuronal subcompartments. Investigations on both invertebrate and vertebrate model systems have revealed local roles for enzymes that attach ubiquitin to substrate proteins, as well as for enzymes that remove ubiquitin from substrates. The proteasome also has been shown to possess disparate functions in different parts of the neuron. Here I give a broad overview of the role of the UPP in synaptic plasticity and highlight the local roles and regulation of the proteolytic pathway in neurons.

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Section: Dubssupporting

confidence: 67%

The ubiquitin-proteasome pathway and synaptic plasticity

Hegde¹

2010

Learn. Mem.

131

123

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“…Ubiquitination has previously been implicated in the cell survival response under conditions of stress, morphogenesis, organogenesis, and exocytosis. It has also been shown to be important in hippocampal long-term potentiation in mice [19] and in the growth of presynaptic nerve terminals in Drosophila [20]. This is interesting because the present studies also showed upregulation of the annexin V protein, which has been shown to have neurotrophic effects on cultured neurons [11].…”

Section: Discussionsupporting

confidence: 68%

Multiplex proteomic analysis by two‐dimensional differential in‐gel electrophoresis

et al. 2003

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This paper describes the use of fluorescence two-dimensional differential in-gel electrophoresis in a multiplex analysis of two distinct proteomes. As a model system, cerebral cortex tissues were analyzed from neurokinin1 receptor knockout (NK 1 R2/2) and wild type (NK 1 R1/1) mice in an attempt to identify molecular pathways involved in the function of this protein. Paired NK 1 R2/2 and NK 1 R1/1 samples were labeled with fluorescent Cy3 and Cy5 dyes and electrophoresed on the same two-dimensional gels. Scanning the gels at wavelengths specific for each dye revealed the two different proteomes which were overlaid and the differences in abundance of specific protein spots were determined by the Amersham Biosciences DeCyder Differential In-gel Analysis software. A Cy2-labeled sample pool was co-electrophoresed with all Cy3-and Cy5-labeled sample pairs as an internal standard providing a link for inter-gel comparisons and for more robust statistical analysis of the data. Eight spots were found to be upregulated and two downregulated in the NK 1 R2/2 mice compared to NK 1 R1/1 controls. Matrix assisted laser desorption/ionisation-time of flight (MALDI-TOF) mass fingerprinting was used to identify the proteins. The results illustrate the power of this multiplex proteomics technology and illustrate how proteomics can be used to understand gene function.

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“…The following flies were used: fmi E59 , UAS-Fmi, UAS-ÎEx (28), Df(2R)stan 2 , fmi 72 (34), elav-Gal4 (DiAntonio et al, 2001), fmi 1071 and fmi 1127 . fmi mutant alleles and the deficiency line were balanced with CyO KrGFP allowing easy selection of GFP-negative fmi mutant larvae (Gao et al, 2000).…”

Section: Fly Strains and Geneticsmentioning

confidence: 99%

“…Other molecules are more directly involved in synaptogenesis, synaptic growth, or maintenance. These molecules include bone morphogenetic protein (Alberle et al, 2002;Marques et al, 2002;Rawson et al, 2003;McCabe et al, 2003;Keshishian and Kim, 2004), ubiquitin (Oh et al, 1994;DiAntonio et al, 2001;Murphey and Godenschwege, 2002;DiAntonio and Hicke, 2004), cell adhesion molecules (Washbourne et al, 2004), and Wingless signaling components (Packard et al, 2003;Charron and Tessier-Lavigne, 2005).…”

Section: Introductionmentioning

confidence: 99%

The atypical cadherin flamingo regulates synaptogenesis and helps prevent axonal and synaptic degeneration in Drosophila

Bao

Berlanga

Xue

et al. 2007

Molecular and Cellular Neuroscience

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The formation of synaptic connections with target cells and maintenance of axons are highly regulated and crucial for neuronal function. The atypical cadherin and G-protein-coupled receptor Flamingo and its orthologs in amphibians and mammals have been shown to regulate cell polarity, dendritic and axonal growth, and neural tube closure. However, the role of Flamingo in synapse formation and function and in axonal health remains poorly understood. Here we show that fmi mutations cause a significant increase in the number of ectopic synapses on muscles and result in the formation of novel en passant synapses along axons, and unique presynaptic varicosities, including active zones, within axons. fmi mutations also cause defective synaptic responses in a small subset of muscles, an agedependent loss of muscle innervation and a drastic degeneration of axons in 3 rd instar larvae without an apparent loss of neurons. Neuronal expression of Flamingo rescues all of these synaptic and axonal defects and larval lethality. Based on these observations, we propose that Flamingo is required in neurons for synaptic target selection, synaptogenesis, the survival of axons and synapses, and adult viability. These findings shed new light on a possible role for Flamingo in progressive neurodegenerative diseases.

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Ubiquitination-dependent mechanisms regulate synaptic growth and function

Cited by 366 publications

References 23 publications

The ubiquitin-proteasome pathway and synaptic plasticity

The ubiquitin-proteasome pathway and synaptic plasticity

Multiplex proteomic analysis by two‐dimensional differential in‐gel electrophoresis

The atypical cadherin flamingo regulates synaptogenesis and helps prevent axonal and synaptic degeneration in Drosophila

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